Transcription Factor 4 Loss-of-function is Associated with Deficits in Progenitor Proliferation and Cortical Neuron Content

Overview

Journal Nat Commun

Specialty Biology

Date 2022 May 2

PMID 35501322

Authors

Fabio Papes

Antonio P Camargo

Janaina S de Souza

Vinicius M A Carvalho

Ryan A Szeto

Erin LaMontagne

Jose R Teixeira

Simoni H Avansini

Sandra M Sanchez-Sanchez

Thiago S Nakahara

Carolina N Santo

Wei Wu

Hang Yao

Barbara M P Araujo

Paulo E N F Velho

Gabriel G Haddad

Alysson R Muotri

Affiliations

Soon will be listed here.

Abstract

Transcription Factor 4 (TCF4) has been associated with autism, schizophrenia, and other neuropsychiatric disorders. However, how pathological TCF4 mutations affect the human neural tissue is poorly understood. Here, we derive neural progenitor cells, neurons, and brain organoids from skin fibroblasts obtained from children with Pitt-Hopkins Syndrome carrying clinically relevant mutations in TCF4. We show that neural progenitors bearing these mutations have reduced proliferation and impaired capacity to differentiate into neurons. We identify a mechanism through which TCF4 loss-of-function leads to decreased Wnt signaling and then to diminished expression of SOX genes, culminating in reduced progenitor proliferation in vitro. Moreover, we show reduced cortical neuron content and impaired electrical activity in the patient-derived organoids, phenotypes that were rescued after correction of TCF4 expression or by pharmacological modulation of Wnt signaling. This work delineates pathological mechanisms in neural cells harboring TCF4 mutations and provides a potential target for therapeutic strategies for genetic disorders associated with this gene.

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